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Fig. 4. Independent confirmation of the adverse effects of unregulated Wnt
signaling in developing stomach endoderm. Findings in E18.5
ShhCre/+;Catnb+/lox(ex3) mouse embryos.
(A,B) Constitutive ß-catenin activation is confirmed by its
nuclear staining (A), compared with membrane staining in areas that escaped
Cre-mediated recombination (B). (C-E) The stomach is reduced in size
and lined by a crowded, villiform epithelium (C,E; H&E stain) that shares
features seen in Barx1 mutant stomach, including thick folds and
mucosal invasion of the mesenchymal layer (E), which contrasts with relatively
normal squamous differentiation (D) in many areas. (F) Radial asymmetry
of E18.5 ShhCre/+;Catnb+/lox(ex3) esophagus,
with squamous (blue arrowheads) and cuboidal (green arrowheads) epithelia on
opposite surfaces. (G) Magnification of the area boxed in F. PAS
staining reveals many cells abnormally producing mucin in the cuboidal
epithelium of the esophagus. (H-J) Although intestinal villi are
absent, there is considerable and ectopic expression of the intestinal marker
Cdx2 (H,I), which is normally excluded from the squamous (J) and glandular
(data not shown) stomach. H is a magnification of the area boxed in C.
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